1. MyD88 Expression by CNS-Resident Cells is Pivotal for Eliciting Protective Immunity in Brain Abscesses
- Author
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Nirmal K. Phulwani, Amy Aldrich, Nilufer Esen, William H. Wood, Mohsin Md. Syed, Sarita Garg, Kevin G. Becker, Tammy Kielian, Yongqing Zhang, Shuliang Liu, and Jessica R. Nichols
- Subjects
TNF-α, tumour necrosis factor-α ,Pfc, complement factor properdin ,0302 clinical medicine ,GFP, green fluorescent protein ,SOCS3, suppressor of cytokine signalling 3 ,0303 health sciences ,Toll-like receptor ,Ier3/IEX, immediate early response 3 ,IL-1R etc., IL-1 receptor ,General Neuroscience ,3. Good health ,brain abscess ,medicine.anatomical_structure ,GAPDH, glyceraldehyde-3-phosphate dehydrogenase ,NF-κB, nuclear factor κB ,medicine.symptom ,Research Article ,TLR, Toll-like receptor ,Staphylococcus aureus ,bone marrow chimaera mice ,Central nervous system ,S7 ,Inflammation ,Biology ,CNS, central nervous system ,S5 ,lcsh:RC321-571 ,Pacsin3, protein kinase C and casein kinase substrate in neurons 3 ,03 medical and health sciences ,ROS, reactive oxygen species ,Immune system ,Immunity ,medicine ,Brain abscess ,lcsh:Neurosciences. Biological psychiatry. Neuropsychiatry ,030304 developmental biology ,KO, knockout ,Innate immune system ,central nervous system ,MyD88 ,medicine.disease ,WT, wild-type ,CFU, colony forming unit ,qRT-PCR, quantitative real-time RT (reverse transcriptase)-PCR ,IL, interleukin ,Immunology ,Neurology (clinical) ,Bone marrow ,Lcn2, lipocalin-2 ,030217 neurology & neurosurgery - Abstract
MyD88 KO (knockout) mice are exquisitely sensitive to CNS (central nervous system) infection with Staphylococcus aureus, a common aetiological agent of brain abscess, exhibiting global defects in innate immunity and exacerbated tissue damage. However, since brain abscesses are typified by the involvement of both activated CNS-resident and infiltrating immune cells, in our previous studies it has been impossible to determine the relative contribution of MyD88-dependent signalling in the CNS compared with the peripheral immune cell compartments. In the present study we addressed this by examining the course of S. aureus infection in MyD88 bone marrow chimaera mice. Interestingly, chimaeras where MyD88 was present in the CNS, but not bone marrow-derived cells, mounted pro-inflammatory mediator expression profiles and neutrophil recruitment equivalent to or exceeding that detected in WT (wild-type) mice. These results implicate CNS MyD88 as essential in eliciting the initial wave of inflammation during the acute response to parenchymal infection. Microarray analysis of infected MyD88 KO compared with WT mice revealed a preponderance of differentially regulated genes involved in apoptotic pathways, suggesting that the extensive tissue damage characteristic of brain abscesses from MyD88 KO mice could result from dysregulated apoptosis. Collectively, the findings of the present study highlight a novel mechanism for CNS-resident cells in initiating a protective innate immune response in the infected brain and, in the absence of MyD88 in this compartment, immunity is compromised.
- Published
- 2009